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Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood

Profiling amino acids and acylcarnitines in whole blood spots is a powerful tool in the laboratory diagnosis of several inborn errors of metabolism. Emerging data suggests that altered blood levels of amino acids and acylcarnitines are also associated with common metabolic diseases in adults. Thus,...

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Autores principales: Burkhardt, Ralph, Kirsten, Holger, Beutner, Frank, Holdt, Lesca M., Gross, Arnd, Teren, Andrej, Tönjes, Anke, Becker, Susen, Krohn, Knut, Kovacs, Peter, Stumvoll, Michael, Teupser, Daniel, Thiery, Joachim, Ceglarek, Uta, Scholz, Markus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4581711/
https://www.ncbi.nlm.nih.gov/pubmed/26401656
http://dx.doi.org/10.1371/journal.pgen.1005510
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author Burkhardt, Ralph
Kirsten, Holger
Beutner, Frank
Holdt, Lesca M.
Gross, Arnd
Teren, Andrej
Tönjes, Anke
Becker, Susen
Krohn, Knut
Kovacs, Peter
Stumvoll, Michael
Teupser, Daniel
Thiery, Joachim
Ceglarek, Uta
Scholz, Markus
author_facet Burkhardt, Ralph
Kirsten, Holger
Beutner, Frank
Holdt, Lesca M.
Gross, Arnd
Teren, Andrej
Tönjes, Anke
Becker, Susen
Krohn, Knut
Kovacs, Peter
Stumvoll, Michael
Teupser, Daniel
Thiery, Joachim
Ceglarek, Uta
Scholz, Markus
author_sort Burkhardt, Ralph
collection PubMed
description Profiling amino acids and acylcarnitines in whole blood spots is a powerful tool in the laboratory diagnosis of several inborn errors of metabolism. Emerging data suggests that altered blood levels of amino acids and acylcarnitines are also associated with common metabolic diseases in adults. Thus, the identification of common genetic determinants for blood metabolites might shed light on pathways contributing to human physiology and common diseases. We applied a targeted mass-spectrometry-based method to analyze whole blood concentrations of 96 amino acids, acylcarnitines and pathway associated metabolite ratios in a Central European cohort of 2,107 adults and performed genome-wide association (GWA) to identify genetic modifiers of metabolite concentrations. We discovered and replicated six novel loci associated with blood levels of total acylcarnitine, arginine (both on chromosome 6; rs12210538, rs17657775), propionylcarnitine (chromosome 10; rs12779637), 2-hydroxyisovalerylcarnitine (chromosome 21; rs1571700), stearoylcarnitine (chromosome 1; rs3811444), and aspartic acid traits (chromosome 8; rs750472). Based on an integrative analysis of expression quantitative trait loci in blood mononuclear cells and correlations between gene expressions and metabolite levels, we provide evidence for putative causative genes: SLC22A16 for total acylcarnitines, ARG1 for arginine, HLCS for 2-hydroxyisovalerylcarnitine, JAM3 for stearoylcarnitine via a trans-effect at chromosome 1, and PPP1R16A for aspartic acid traits. Further, we report replication and provide additional functional evidence for ten loci that have previously been published for metabolites measured in plasma, serum or urine. In conclusion, our integrative analysis of SNP, gene-expression and metabolite data points to novel genetic factors that may be involved in the regulation of human metabolism. At several loci, we provide evidence for metabolite regulation via gene-expression and observed overlaps with GWAS loci for common diseases. These results form a strong rationale for subsequent functional and disease-related studies.
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spelling pubmed-45817112015-10-01 Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood Burkhardt, Ralph Kirsten, Holger Beutner, Frank Holdt, Lesca M. Gross, Arnd Teren, Andrej Tönjes, Anke Becker, Susen Krohn, Knut Kovacs, Peter Stumvoll, Michael Teupser, Daniel Thiery, Joachim Ceglarek, Uta Scholz, Markus PLoS Genet Research Article Profiling amino acids and acylcarnitines in whole blood spots is a powerful tool in the laboratory diagnosis of several inborn errors of metabolism. Emerging data suggests that altered blood levels of amino acids and acylcarnitines are also associated with common metabolic diseases in adults. Thus, the identification of common genetic determinants for blood metabolites might shed light on pathways contributing to human physiology and common diseases. We applied a targeted mass-spectrometry-based method to analyze whole blood concentrations of 96 amino acids, acylcarnitines and pathway associated metabolite ratios in a Central European cohort of 2,107 adults and performed genome-wide association (GWA) to identify genetic modifiers of metabolite concentrations. We discovered and replicated six novel loci associated with blood levels of total acylcarnitine, arginine (both on chromosome 6; rs12210538, rs17657775), propionylcarnitine (chromosome 10; rs12779637), 2-hydroxyisovalerylcarnitine (chromosome 21; rs1571700), stearoylcarnitine (chromosome 1; rs3811444), and aspartic acid traits (chromosome 8; rs750472). Based on an integrative analysis of expression quantitative trait loci in blood mononuclear cells and correlations between gene expressions and metabolite levels, we provide evidence for putative causative genes: SLC22A16 for total acylcarnitines, ARG1 for arginine, HLCS for 2-hydroxyisovalerylcarnitine, JAM3 for stearoylcarnitine via a trans-effect at chromosome 1, and PPP1R16A for aspartic acid traits. Further, we report replication and provide additional functional evidence for ten loci that have previously been published for metabolites measured in plasma, serum or urine. In conclusion, our integrative analysis of SNP, gene-expression and metabolite data points to novel genetic factors that may be involved in the regulation of human metabolism. At several loci, we provide evidence for metabolite regulation via gene-expression and observed overlaps with GWAS loci for common diseases. These results form a strong rationale for subsequent functional and disease-related studies. Public Library of Science 2015-09-24 /pmc/articles/PMC4581711/ /pubmed/26401656 http://dx.doi.org/10.1371/journal.pgen.1005510 Text en © 2015 Burkhardt et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Burkhardt, Ralph
Kirsten, Holger
Beutner, Frank
Holdt, Lesca M.
Gross, Arnd
Teren, Andrej
Tönjes, Anke
Becker, Susen
Krohn, Knut
Kovacs, Peter
Stumvoll, Michael
Teupser, Daniel
Thiery, Joachim
Ceglarek, Uta
Scholz, Markus
Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood
title Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood
title_full Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood
title_fullStr Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood
title_full_unstemmed Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood
title_short Integration of Genome-Wide SNP Data and Gene-Expression Profiles Reveals Six Novel Loci and Regulatory Mechanisms for Amino Acids and Acylcarnitines in Whole Blood
title_sort integration of genome-wide snp data and gene-expression profiles reveals six novel loci and regulatory mechanisms for amino acids and acylcarnitines in whole blood
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4581711/
https://www.ncbi.nlm.nih.gov/pubmed/26401656
http://dx.doi.org/10.1371/journal.pgen.1005510
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